Psychosis Clinical Trial
Official title:
Prevention Trial of Family Focused Treatment in Youth at Risk for Psychosis
Preventing psychotic disorders such as schizophrenia and associated functional disability could relieve an enormous burden of personal and family suffering and economic losses to society. This project aims to conduct a pilot randomized trial to determine the efficacy of a family-focused treatment in comparison with treatment-as-usual in enhancing functional outcomes, stabilizing symptoms, and preventing or delaying the onset of full psychosis in transitional age youth with prodromal symptoms. The results of this study will be crucial for the development of cost-effective, evidence-based psychosocial approaches to psychosis prevention and thus will have major implications for public health.
The goal of this research is to conduct a multisite randomized trial to determine the
efficacy of a 6-month Family-Focused Treatment (FFT) in comparison with Enhanced Care (EC),
a treatment-as-usual intervention, in reducing symptoms, enhancing functional outcomes, and
preventing or delaying the onset of full psychosis in youth aged 12-35 years who meet
criteria for a prodromal risk syndrome according to the Structured Interview for Prodromal
Syndromes (SIPS). Our primary, secondary, and tertiary hypotheses, respectively, are that
at-risk probands will respond better to FFT than EC at 6- and 12-month follow-ups, in terms
of symptom trajectories (SIPS scores), social/family functioning, and first onset of full
psychosis. Subjects will be drawn from the participants in a prospective, longitudinal study
elucidating predictors and mechanisms of conversion to psychosis (North American Prodrome
Longitudinal Study, or NAPLS), on which the sites collaborate. Subjects will be interviewed
every 6 months for 1 year to assess positive and negative symptoms, academic and social
functioning, family functioning, and conversion to psychosis.
Recent progress in risk ascertainment methodology has enabled reliable identification of
persons with prodromal or "clinical high-risk" syndromes, 35% of whom develop psychosis
within 2 and ½ years. This paradigm provides an opportunity for developing and testing
interventions in the prodromal phase, before the onset of full psychosis and accumulation of
substantial functional disability. Psychosocial interventions appear to be well suited to
address issues of motivational deficits and functional disability in the psychosis prodrome.
Given our present state of knowledge regarding the mechanisms of psychosis onset, and given
that initial studies of antipsychotic drugs in prodromal patients have produced discouraging
results in terms of prevention, a short term reduction in symptom severity and functional
disability may represent a more achievable target than a reduction in psychosis incidence.
We have developed and piloted a version of FFT for clinical high risk youth (FFT-CHR)
consisting of psychoeducation, communication training, and problem-solving skills training.
In randomized trials, adults and adolescents with bipolar disorder and children at-risk for
bipolar disorder undergoing FFT improved symptomatically and functionally compared to
patients in brief psychoeducational control conditions. Further, an open trial of family
psychoeducation for youth at risk for psychosis demonstrated symptomatic and functional
improvements relative to baseline scores. However, no randomized controlled study has
examined the efficacy of FFT for reducing symptoms or functional disability in youth at risk
for psychosis.
In view of the improvements in quality of life and the reductions in costs of care that have
occurred with preventive approaches to cardiovascular disease, diabetes, and certain forms
of cancer, the field of psychiatry is in need of a major commitment to an early
detection/prevention framework for its most debilitating syndromes - the psychotic
disorders. The prodromal risk syndrome criteria have resulted in clinical algorithms that
are highly effective in predicting onset of full psychosis. However, such knowledge will be
of limited utility if we lack the means of intervening in the pre-onset phase in a way that
either reduces the likelihood of progression to full psychosis, the accumulation of
functional disability, or both. There are currently no cost-effective, evidence-based
psychosocial approaches to psychosis prevention. Preventing the neurotoxic effects of early
episodes, before these illnesses become chronic, and minimizing the psychosocial sequelae of
early episodes, may do much to prevent the long-term disability caused by psychosis and
thereby have a major impact on public health. Our study will take the critical next step by
performing an initial efficacy test of a highly promising family-focused intervention
designed to stabilize symptoms and improve social and role functioning in at risk youth.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Factorial Assignment, Masking: Single Blind (Outcomes Assessor), Primary Purpose: Treatment
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